Virulence and pathogenicity of three Trypanosoma brucei rhodesiense stabilates in a Swiss white mouse model

African Journal of Laboratory Medicine

 
 
Field Value
 
Title Virulence and pathogenicity of three Trypanosoma brucei rhodesiense stabilates in a Swiss white mouse model
 
Creator Kariuki, Christopher Kagira, John M. Mwadime, Victor Ngotho, Maina
 
Subject — —
Description Background: A key objective in basic research on human African trypanosomiasis (HAT) is developing a cheap and reliable experimental model of the disease for use in pathogenesis and drug studies.Objective: With a view to improving current models, a study was undertaken to characterise the virulence and pathogenicity of three Trypanosoma brucei rhodesiense stabilates, labelled as International Livestock Research Institute (ILRI)-2918, ILRI-3953, and Institute of Primate Research (IPR)-001, infected into Swiss white mice.Methods: Swiss white mice were infected intraperitoneally with trypanosomes and observedfor parasitaemia using wet blood smears obtained by tail snipping. Induction of late-stagedisease was undertaken using diminazene aceturate (40 mg/kg, Berenil) with curativetreatment done using melarsoprol (3.6 mg/kg, Arsobal).Results: The prepatent period for the stabilates ranged from three to four days with mean peak parasitaemia ranging from Log10 6.40 to 8.36. First peak parasitaemia for all stabilates varied between six and seven days post infection (DPI) followed by secondary latency in ILRI-2918 (15–17 DPI) and IPR-001 (17–19 DPI). Survival times ranged from six DPI (ILRI-3953) to 86 DPI (IPR-001). Hindleg paresis was observed in both ILRI-3953 (at peak parasitaemia) and ILRI-2918 (after relapse parasitaemia). Mice infected with IPR-001 survived until 54 DPI when curative treatment was undertaken.Conclusions: This study demonstrated that the stabilates ILRI-2918 and ILRI-3953 were unsuitable for modelling late-stage HAT in mice. The stabilate IPR-001 demonstrated the potential to induce chronic trypanosomiasis in Swiss white mice for use in development of a late-stage model of HAT.
 
Publisher AOSIS
 
Contributor Institute of Primate Research
Date 2015-10-05
 
Type info:eu-repo/semantics/article info:eu-repo/semantics/publishedVersion — —
Format text/html application/octet-stream text/xml application/pdf
Identifier 10.4102/ajlm.v4i1.137
 
Source African Journal of Laboratory Medicine; Vol 4, No 1 (2015); 8 pages 2225-2010 2225-2002
 
Language eng
 
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https://ajlmonline.org/index.php/ajlm/article/view/137/398 https://ajlmonline.org/index.php/ajlm/article/view/137/399 https://ajlmonline.org/index.php/ajlm/article/view/137/400 https://ajlmonline.org/index.php/ajlm/article/view/137/386
 
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Rights Copyright (c) 2015 Christopher Kariuki, John M. Kagira, Victor Mwadime, Maina Ngotho https://creativecommons.org/licenses/by/4.0
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